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首页> 外文期刊>DNA repair >The archaeal Xpf/Mus81/FANCM homolog Hef and the Holliday junction resolvase Hjc define alternative pathways that are essential for cell viability in Haloferax volcanii.
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The archaeal Xpf/Mus81/FANCM homolog Hef and the Holliday junction resolvase Hjc define alternative pathways that are essential for cell viability in Haloferax volcanii.

机译:古老的Xpf / Mus81 / FANCM同源物Hef和Holliday联结解析酶Hjc定义了对于Haloferax volcanii细胞活力至关重要的替代途径。

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摘要

The XPF/MUS81 family of endonucleases is found in eukaryotes and archaea, in the former they play a critical role in DNA repair and replication fork restart. Hef is a XPF/MUS81 family member found in Euryarchaea and is related to the Fanconi anemia protein FANCM. We have studied the role of Hef in the euryarchaeon Haloferax volcanii. Unlike Xpf in eukaryotes, Hef is not involved in nucleotide excision repair; instead, this function is encoded by the uvrABC genes. Similarly, deletion of hef confers only moderate sensitivity to DNA crosslinking agents, whereas mutation of FANCM in leads to hypersensitivity in eukaryotes. However, Hef is essential for cell viability when the Holliday junction resolvase Hjc is absent, and both the helicase and nuclease activities of Hef are indispensable. By contrast, single mutants of hjc and hef display no significant defects in growth or homologous recombination. This suggests that Hef and Hjc are redundant for the resolution of recombination intermediates, and that Hef is the functional homolog of eukaryotic Mus81. Furthermore, deletion of hef in a recombination-deficient DeltaradA background is highly deleterious but deletion of hjc has no effect. Therefore, Hjc acts exclusively in homologous recombination whereas Hef, in addition to its role in resolving recombination intermediates, can act in a pathway that avoids the use of homologous recombination. We propose that Hef and Hjc provide alternative means to restart stalled DNA replication forks.
机译:XPF / MUS81内切核酸酶家族存在于真核生物和古细菌中,前者在DNA修复和复制叉重启中起关键作用。 Hef是在Euryarchaea中发现的XPF / MUS81家族成员,与Fanconi贫血蛋白FANCM有关。我们已经研究了Hef在euryarchaeon Haloferax volcanii中的作用。与真核生物中的Xpf不同,Hef不参与核苷酸切除修复。相反,此功能由uvrABC基因编码。类似地,hef的缺失仅赋予对DNA交联剂中等的敏感性,而FANCM的突变导致真核生物的超敏感性。但是,当缺少霍利迪连接解酶Hjc时,Hef对于细胞生存力至关重要,Hef的解旋酶和核酸酶活性都是必不可少的。相反,hjc和hef的单个突变体在生长或同源重组中没有显示出明显的缺陷。这表明Hef和Hjc对于重组中间体的分离是多余的,并且Hef是真核Mus81的功能同源物。此外,在缺乏重组的DeltaradA背景中删除hef具有很高的有害性,但是删除hjc无效。因此,Hjc仅在同源重组中起作用,而Hef除了在解析重组中间体中的作用外,还可以在避免使用同源重组的途径中起作用。我们建议Hef和Hjc提供重新启动停滞的DNA复制叉的替代方法。

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